Palindromic Rheumatism As Part of the Rheumatoid Arthritis Continuum

Palindromic Rheumatism As Part of the Rheumatoid Arthritis Continuum

This is a repository copy of Palindromic rheumatism as part of the rheumatoid arthritis continuum. White Rose Research Online URL for this paper: http://eprints.whiterose.ac.uk/147742/ Version: Accepted Version Article: Mankia, K and Emery, P orcid.org/0000-0002-7429-8482 (2019) Palindromic rheumatism as part of the rheumatoid arthritis continuum. Nature Reviews Rheumatology, 15 (11). pp. 687-695. ISSN 1759-4790 https://doi.org/10.1038/s41584-019-0308-5 © 2019, Springer Nature. This is an author produced version of a journal article published in Nature Reviews Rheumatology. Uploaded in accordance with the publisher's self-archiving policy. Reuse Items deposited in White Rose Research Online are protected by copyright, with all rights reserved unless indicated otherwise. They may be downloaded and/or printed for private study, or other acts as permitted by national copyright laws. The publisher or other rights holders may allow further reproduction and re-use of the full text version. This is indicated by the licence information on the White Rose Research Online record for the item. Takedown If you consider content in White Rose Research Online to be in breach of UK law, please notify us by emailing [email protected] including the URL of the record and the reason for the withdrawal request. [email protected] https://eprints.whiterose.ac.uk/ Perspective How does Palindromic Rheumatism fit into the Rheumatoid Arthritis Continuum? Kulveer Mankia1,2 & Paul Emery1,2 1. Leeds Institute of Rheumatic and Musculoskeletal Medicine, University of Leeds, Leeds, UK 2. NIHR Leeds Biomedical Research Centre, Leeds Teaching Hospitals NHS Trust, Chapel Allerton Hospital, Leeds, UK Abstract Palindromic rheumatism (PR) is a distinctive syndrome which has a long-recognised association with rheumatoid arthritis (RA). PR is characterised by intermittent flares of pain, erythema and swelling in and around the joints, which are typically severe and unpredictable. The observation that most PR patients have RA-related autoantibodies and that many eventually develop RA has led to PR often being viewed as a relapsing-remitting variant of RA. However, the clinical and imaging phenotypes of PR suggest important distinctions from RA and imply underlying mechanistic differences between the two conditions. Furthermore, there are interesting parallels between the pattern of inflammation seen in PR with that seen in other groups of symptomatic individuals at risk of RA development. In this article we will explore the concept of PR as part of the RA continuum and propose an updated disease paradigm for this unique syndrome. 1 Introduction Palindromic rheumatism (PR) is a clinical syndrome characterised by debilitating flares of pain, swelling and erythema centred around the joints. PR is encountered by most rheumatologists in routine clinical practice, yet the diagnosis can be challenging and the pathogenesis and optimal treatments are unclear. Patients with PR often go on to develop rheumatoid arthritis (RA). The shared risk factors, including genetics and autoantibodies, and the typical distribution of affected joints, suggest PR may be a relapsing-remitting form of RA, which progresses to persistent disease. However, the flares that define PR are not typical of an autoimmune phenotype but appear to be more closely related to an autoinflammatory process (see later for explanation). In this article we will focus on the unique phenotype of PR and its relationship with RA. We will describe the similarities between PR and RA prodromes and what this tells us about RA pathogenesis. Finally we will outline an overarching hypothesis for PR and explore how this may refine the management of this curious syndrome. Is PR simply relapsing-remitting RA? Conventional wisdom tells us that PR is closely associated with RA. This is largely based on observations of the natural history and the clinical and serological features of this syndrome. The authors of some of the earliest clinical studies of PR reported high rates of progression to RA in their respective PR cohorts (1-4). In the first longitudinal study of PR, Ansell and Bywaters reported progression to RA in 18/28 (64%) patients within 8 years of follow up (1). Subsequently, high rates of progression were also reported in two other UK cohorts; Mattingly observed 10 of 20 PR patients developed RA over 10 years of follow up 2 (2), while Wajed et al reported progression to RA in 17/39 (44%) of their patients (3). Similarly, in a Finnish cohort, Hannonen et al described progression to persistent arthritis in 35/60 (58%) PR patients (4). Based on these observations, most investigators proposed that PR represents an atypical, relapsing-remitting form of RA and if patients were followed up for long enough, the development of full-blown RA would be inevitable for most. Indeed, when the Finnish PR cohort described by Hannonen et al was re-examined after over twenty years of follow up, two-thirds of all patients had developed RA, with all but two patients having progressed within the first 10 years of follow up (5). A further argument for a close association between PR and RA is the two conditions have a similar prevalence of RA-related autoantibodies. A high prevalence of rheumatoid factor positivity was identified in early PR studies, prior to the availability of anti-citrullinated protein antibody (ACPA) testing (3, 4) . In a cross-sectional analysis of a Spanish PR cohort, the frequency of anti-CCP antibodies was similar in PR compared with early RA patients (53% vs 55% respectively) (6). Other international PR cohorts report similarly high frequencies of anti-CCP positivity (between 46% and 68%) (7-11). A notable outlier is a recently described Taiwanese PR cohort where only 11/84 (13%) of patients were anti-CCP positive and 12/84 (14%) were RF positive (12). Variable inclusion criteria, recruitment strategies, geographical differences in patient profiles and possible pathogens could all explain the apparent disparity in these data. There is also evidence of immunogenetic similarity between PR and RA. The initial genetic studies in PR were performed in relatively small groups of patients and used serological rather than DNA typing for HLA antigens, producing mixed results (13-16). However, in a larger more recent study, an increased prevalence of HLA-DR shared epitope (SE) alleles in 3 PR patients compared with controls was reported (17). That study found homozygosity of SE alleles to be predictive of progression to chronic arthritis, although SE status was not found to be as predictive in a subsequent smaller study of Japanese PR patients (8). Thus the immunogenetic and serological profile of PR, added to its propensity to become full-blown RA suggests it could be considered as a relapsing-remitting form of RA, which, over time, naturally progresses from an intermittent to a persistent arthritis. For this to be true, one would expect the pattern of joint inflammation in flares of PR to be similar to that seen in RA. However, a recent imaging study of treatment-naïve PR patients observed the opposite (11). PR flares were characterised by a high frequency of extra- capsular inflammation on ultrasound (US); 61% of patients had this finding and interestingly in 63% of these cases there was no co-existent synovitis. In contrast, only 23% of patients had evidence of US synovitis during flare. Isolated extra-capsular inflammation appeared to distinguish PR from RA as this pattern was rarely seen in the RA patients. As may be expected, US inflammation was rarely seen in PR patients when they were not flaring (11). These new data suggest PR is not in fact characterised by relapsing-remitting synovitis but instead by a different pattern of inflammation, focused on peri-articular rather than intra- articular structures (figure 1). Is PR a distinct disease entity? Despite the shared genetic and immunological risk factors, the distinct pattern of inflammation in PR suggests the notion of this syndrome as a relapsing-remitting prodrome of RA may be an oversimplification. Indeed, a minority of PR patients will go on to develop other chronic diseases, e.g. connective tissue disorders or vasculitis and not necessarily RA 4 (4, 18). Furthermore, seropositive and seronegative PR may be mechanistically and phenotypically distinct. While there is little published data that directly addresses this, the genetic and immunological risk factors that link PR and RA are clearly specific to seropositive disease. It is therefore possible that seronegative PR is more genetically and phenotypically heterogeneous. This is certainly an area which warrants further exploration. The evidence for distinct disease mechanisms in PR will now be discussed in the context of clinical features, genetics, imaging findings and response to treatment. Clinical features PR and RA have a predilection for the same joints. Studies of different PR cohorts have consistently reported the wrists, metacarpophalangeal joints (MCPJs) and proximal interphalangeal joints (PIPJs) as the most commonly affected sites in PR (2, 4, 8, 9, 19, 20). In contrast, the spine and sternoclavicular joints are the least frequently affected sites (mean 4% and 2% of patients respectively) (19). However, despite the distribution of affected joints being similar, the nature of the inflammation seen in these syndromes appears to be different. Painful inflammatory flares are the hallmark of PR and are frequently characterised by peri-articular soft tissue inflammation (19). Indeed, in the original description of PR, Hench and Rosenberg chose the name palindromic palindromic based on the striking peri-arthritis and para-arthritis observed in some of their patients (20). Subsequent clinical descriptions have confirmed peri-articular involvement and skin erythema as typical clinical signs of PR (2, 19). Whether peri-articular inflammation occurs in the presence or absence of co-existent synovitis is difficult to establish on clinical examination alone and requires high resolution imaging (see below).

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